Jossin Yves, Ogawa Masuhara, Metin Christine, Tissir Fadel, Goffinet André M
University of Louvain Medical School, Developmental Genetics Unit, GEDE 7382, B1200 Brussels, Belgium.
J Neurosci. 2003 Oct 29;23(30):9953-9. doi: 10.1523/JNEUROSCI.23-30-09953.2003.
During development, most cortical neurons migrate to the cortical plate (CP) radially. CP development is abnormal in reeler and other mutant mice with defective Reelin signaling. Reelin is secreted by Cajal-Retzius cells and binds to the very low density lipoprotein receptor and apolipoprotein E receptor type 2 receptors on the surface of CP cells, inducing tyrosine phosphorylation of the intracellular Dab1 adapter. As with Reelin receptors, the identification of Reelin signaling partners is hampered by genetic redundancy. Using a new in vitro embryonic slice culture system, we demonstrate that chemical inhibitors of Src family kinases and Abl, but not inhibitors of Abl alone, generate a reeler-like malformation and that inhibitors of protein kinases C induce a malformation of cortical development that is also reminiscent of reeler. Our observations demonstrate a key role for these enzymes in radial migration to the cortical plate, possibly via interference with Reelin signaling.
在发育过程中,大多数皮质神经元沿径向迁移至皮质板(CP)。在瑞连蛋白信号缺陷的reeler及其他突变小鼠中,CP发育异常。瑞连蛋白由卡哈尔-雷茨细胞分泌,并与CP细胞表面的极低密度脂蛋白受体及载脂蛋白E受体2型受体结合,诱导细胞内衔接蛋白Dab1的酪氨酸磷酸化。与瑞连蛋白受体一样,由于基因冗余,瑞连蛋白信号转导伙伴的鉴定受到阻碍。利用一种新的体外胚胎切片培养系统,我们证明Src家族激酶和Abl的化学抑制剂(而非单独的Abl抑制剂)会产生类似reeler的畸形,蛋白激酶C抑制剂会诱导皮质发育畸形,这也让人联想到reeler。我们的观察结果表明,这些酶在向皮质板的径向迁移中可能通过干扰瑞连蛋白信号发挥关键作用。